Blocking CTLA-4 while priming with a whole cell vaccine reshapes the oligoclonal T cell infiltrate and eradicates tumors in an orthotopic glioma model

Blocking CTLA-4 while priming with a whole cell vaccine reshapes the oligoclonal T cell infiltrate and eradicates tumors in an orthotopic glioma model

Vaccine-mediated cancer treatment is unlikely to induce long-term survival unless suppressive mechanisms are overcome. Given the success of antibody-mediated immune checkpoint blockade in relieving regulation of endogenous anti-tumor T cell responses in tumor-burdened hosts, we investigated whether...

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Main Authors: Field, Cameron S., Hunn, Martin K., Ferguson, Peter M., Ruedl, Christiane, Ancelet, Lindsay R., Hermans, Ian F.
Other Authors: School of Biological Sciences
Format: Article
Language:English
Published: 2019
Subjects:
Vaccine
Checkpoint Blockade
Science::Biological sciences
Online Access:https://hdl.handle.net/10356/85533
http://hdl.handle.net/10220/49233
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-855332020-03-07T12:18:10Z Blocking CTLA-4 while priming with a whole cell vaccine reshapes the oligoclonal T cell infiltrate and eradicates tumors in an orthotopic glioma model Field, Cameron S. Hunn, Martin K. Ferguson, Peter M. Ruedl, Christiane Ancelet, Lindsay R. Hermans, Ian F. School of Biological Sciences Vaccine Checkpoint Blockade Science::Biological sciences Vaccine-mediated cancer treatment is unlikely to induce long-term survival unless suppressive mechanisms are overcome. Given the success of antibody-mediated immune checkpoint blockade in relieving regulation of endogenous anti-tumor T cell responses in tumor-burdened hosts, we investigated whether checkpoint blockade could improve the efficacy of responses induced with a whole tumor-cell vaccine. We show that administration of a single dose of blocking antibody was sufficient to significantly enhance antitumor activity of the vaccine, inducing complete radiological regression of established intracranial tumors. The antibody or vaccine alone were ineffective in this setting. The antibody had to be administered before, or close to, vaccine administration, suggesting CTLA-4 blockade had an impact on early priming events. The combined treatment resulted in enhanced trapping of leukocytes in the lymphoid tissues, including T cells that had undergone significant proliferation. There were no obvious changes in the stimulatory function of antigen-presenting cells or the number and function of regulatory T cells, suggesting T cells were the targets of the checkpoint blockade. While tumors regressing under combined treatment were highly infiltrated with a variety of leukocytes, tumor eradication was dependent on CD4+ T cells. Analysis of the TCR repertoire showed that the addition of anti-CTLA-4 at priming reshaped the repertoire of tumor infiltrating T cells. In particular, the oligoclonal populations became greater in magnitude and more diverse in specificity. Using anti-CTLA-4 in a restricted way to promote the priming phase of an anti-cancer vaccine may offer a useful way of harnessing clinical benefit from this powerful agent. 2019-07-10T02:26:47Z 2019-12-06T16:05:29Z 2019-07-10T02:26:47Z 2019-12-06T16:05:29Z 2017 Journal Article Field, C. S., Hunn, M. K., Ferguson, P. M., Ruedl, C., Ancelet, L. R., & Hermans, I. F. (2017). Blocking CTLA-4 while priming with a whole cell vaccine reshapes the oligoclonal T cell infiltrate and eradicates tumors in an orthotopic glioma model. OncoImmunology, 7(1), e1376154-. doi:10.1080/2162402X.2017.1376154 2162-4011 https://hdl.handle.net/10356/85533 http://hdl.handle.net/10220/49233 10.1080/2162402X.2017.1376154 en OncoImmunology © 2018 Taylor & Francis Group, LLC. All rights reserved.
institution Nanyang Technological University
building NTU Library
country Singapore
collection DR-NTU
language English
topic Vaccine
Checkpoint Blockade
Science::Biological sciences
spellingShingle Vaccine
Checkpoint Blockade
Science::Biological sciences
Field, Cameron S.
Hunn, Martin K.
Ferguson, Peter M.
Ruedl, Christiane
Ancelet, Lindsay R.
Hermans, Ian F.
Blocking CTLA-4 while priming with a whole cell vaccine reshapes the oligoclonal T cell infiltrate and eradicates tumors in an orthotopic glioma model
description Vaccine-mediated cancer treatment is unlikely to induce long-term survival unless suppressive mechanisms are overcome. Given the success of antibody-mediated immune checkpoint blockade in relieving regulation of endogenous anti-tumor T cell responses in tumor-burdened hosts, we investigated whether checkpoint blockade could improve the efficacy of responses induced with a whole tumor-cell vaccine. We show that administration of a single dose of blocking antibody was sufficient to significantly enhance antitumor activity of the vaccine, inducing complete radiological regression of established intracranial tumors. The antibody or vaccine alone were ineffective in this setting. The antibody had to be administered before, or close to, vaccine administration, suggesting CTLA-4 blockade had an impact on early priming events. The combined treatment resulted in enhanced trapping of leukocytes in the lymphoid tissues, including T cells that had undergone significant proliferation. There were no obvious changes in the stimulatory function of antigen-presenting cells or the number and function of regulatory T cells, suggesting T cells were the targets of the checkpoint blockade. While tumors regressing under combined treatment were highly infiltrated with a variety of leukocytes, tumor eradication was dependent on CD4+ T cells. Analysis of the TCR repertoire showed that the addition of anti-CTLA-4 at priming reshaped the repertoire of tumor infiltrating T cells. In particular, the oligoclonal populations became greater in magnitude and more diverse in specificity. Using anti-CTLA-4 in a restricted way to promote the priming phase of an anti-cancer vaccine may offer a useful way of harnessing clinical benefit from this powerful agent.
author2 School of Biological Sciences
author_facet School of Biological Sciences
Field, Cameron S.
Hunn, Martin K.
Ferguson, Peter M.
Ruedl, Christiane
Ancelet, Lindsay R.
Hermans, Ian F.
format Article
author Field, Cameron S.
Hunn, Martin K.
Ferguson, Peter M.
Ruedl, Christiane
Ancelet, Lindsay R.
Hermans, Ian F.
author_sort Field, Cameron S.
title Blocking CTLA-4 while priming with a whole cell vaccine reshapes the oligoclonal T cell infiltrate and eradicates tumors in an orthotopic glioma model
title_short Blocking CTLA-4 while priming with a whole cell vaccine reshapes the oligoclonal T cell infiltrate and eradicates tumors in an orthotopic glioma model
title_full Blocking CTLA-4 while priming with a whole cell vaccine reshapes the oligoclonal T cell infiltrate and eradicates tumors in an orthotopic glioma model
title_fullStr Blocking CTLA-4 while priming with a whole cell vaccine reshapes the oligoclonal T cell infiltrate and eradicates tumors in an orthotopic glioma model
title_full_unstemmed Blocking CTLA-4 while priming with a whole cell vaccine reshapes the oligoclonal T cell infiltrate and eradicates tumors in an orthotopic glioma model
title_sort blocking ctla-4 while priming with a whole cell vaccine reshapes the oligoclonal t cell infiltrate and eradicates tumors in an orthotopic glioma model
publishDate 2019
url https://hdl.handle.net/10356/85533
http://hdl.handle.net/10220/49233
_version_ 1681040694952591360

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